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药物靶点通常如此,而具有副作用的药物靶点则尤其会成为人类相互作用组扰动的良好传播者。

Targets of drugs are generally, and targets of drugs having side effects are specifically good spreaders of human interactome perturbations.

作者信息

Perez-Lopez Áron R, Szalay Kristóf Z, Türei Dénes, Módos Dezső, Lenti Katalin, Korcsmáros Tamás, Csermely Peter

机构信息

Department of Medical Chemistry, Semmelweis University, P.O. Box 260, H-1444 Budapest 8, Hungary.

Department of Genetics, Eötvös Loránd University, Pázmány P. s. 1C, H-1117 Budapest, Hungary.

出版信息

Sci Rep. 2015 May 11;5:10182. doi: 10.1038/srep10182.

Abstract

Network-based methods are playing an increasingly important role in drug design. Our main question in this paper was whether the efficiency of drug target proteins to spread perturbations in the human interactome is larger if the binding drugs have side effects, as compared to those which have no reported side effects. Our results showed that in general, drug targets were better spreaders of perturbations than non-target proteins, and in particular, targets of drugs with side effects were also better spreaders of perturbations than targets of drugs having no reported side effects in human protein-protein interaction networks. Colorectal cancer-related proteins were good spreaders and had a high centrality, while type 2 diabetes-related proteins showed an average spreading efficiency and had an average centrality in the human interactome. Moreover, the interactome-distance between drug targets and disease-related proteins was higher in diabetes than in colorectal cancer. Our results may help a better understanding of the network position and dynamics of drug targets and disease-related proteins, and may contribute to develop additional, network-based tests to increase the potential safety of drug candidates.

摘要

基于网络的方法在药物设计中发挥着越来越重要的作用。我们在本文中的主要问题是,与那些没有报道有副作用的药物相比,如果结合药物有副作用,药物靶蛋白在人类相互作用组中传播扰动的效率是否更高。我们的结果表明,一般来说,药物靶点比非靶点蛋白更能有效地传播扰动,特别是在人类蛋白质-蛋白质相互作用网络中,有副作用药物的靶点比没有报道有副作用药物的靶点更能有效地传播扰动。结直肠癌相关蛋白是良好的传播者且具有较高的中心性,而2型糖尿病相关蛋白在人类相互作用组中显示出平均的传播效率和平均的中心性。此外,药物靶点与疾病相关蛋白之间的相互作用组距离在糖尿病中比在结直肠癌中更高。我们的结果可能有助于更好地理解药物靶点和疾病相关蛋白的网络位置及动态,并可能有助于开发更多基于网络的测试,以提高候选药物的潜在安全性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4d7e/4426692/d9c538fe967d/srep10182-f1.jpg

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